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κ-Carrageenan/sericin polymer matrix modified with different crosslinking agents and thermal crosslinking: Improved release profile of mefenamic acid

热重分析 材料科学 聚合物 化学工程 热稳定性 甲芬那酸 傅里叶变换红外光谱 化学 色谱法 复合材料 工程类
作者
Wedja Timóteo Vieira,Maria Vitória Silva Nicolini,Meuris Gurgel Carlos da Silva,Laura de Oliveira Nascimento,Melissa Gurgel Adeodato Vieira
出处
期刊:International Journal of Biological Macromolecules [Elsevier]
卷期号:262: 129823-129823
标识
DOI:10.1016/j.ijbiomac.2024.129823
摘要

The crosslinking of the polymer matrix with compatible macromolecules results in a three-dimensional network structure that offers an enhancement in the controlled release properties of the material. In this sense, this work aimed to improve the release profile of mefenamic acid (MAC) through crosslinking strategies. κ-Carrageenan/sericin crosslinked blend was obtained by covalent and thermal crosslinking and the different formulations were characterized. The gastroresistant potential and release profile were evaluated in the dissolution assay. The effect and characterization of the particles were investigated. Multiple units presented high entrapment efficiency (94.11–104.25), high drug loading (36.50–47.50 %) and adequate particle size (1.34–1.57 mm) with rough surface and visually spherical shape. The Weibull model showed that drug release occurred by relaxation, erosion and Fickian diffusion. Material stability and absence of MAC -polymer interactions were demonstrated by FTIR and thermogravimetric analysis. DSC showed a stable character of MAC in the drug-loaded beads. Moreover, the application studies of κ-Car/Ser/carboxymethylcellulose in the in vitro intestine mode showed that the crosslinked blend increased cell viability (>85 %), while free MAC exhibited a cytotoxic effect. Finally, the crosslinked k-Car/Ser blend MAC -loaded showed promising properties of a sustained release form of anti-inflammatory drug.
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